Department of Pharmaceutical and Biomedical Sciences, College of Pharmacy, The University of Georgia , Athens, Georgia 30602, United States.
J Med Chem. 2014 Mar 27;57(6):2611-22. doi: 10.1021/jm401884z. Epub 2014 Mar 6.
Protein arginine methylation is a posttranslational modification critical for a variety of biological processes. Misregulation of protein arginine methyltransferases (PRMTs) has been linked to many pathological conditions. Most current PRMT inhibitors display limited specificity and selectivity, indiscriminately targeting many methyltransferase enzymes that use S-adenosyl-l-methionine as a cofactor. Here we report diamidine compounds for specific inhibition of PRMT1, the primary type I enzyme. Docking, molecular dynamics, and MM/PBSA analysis together with biochemical assays were conducted to understand the binding modes of these inhibitors and the molecular basis of selective inhibition for PRMT1. Our data suggest that 2,5-bis(4-amidinophenyl)furan (1, furamidine, DB75), one leading inhibitor, targets the enzyme active site and is primarily competitive with the substrate and noncompetitive toward the cofactor. Furthermore, cellular studies revealed that 1 is cell membrane permeable and effectively inhibits intracellular PRMT1 activity and blocks cell proliferation in leukemia cell lines with different genetic lesions.
蛋白质精氨酸甲基化是一种翻译后修饰,对于多种生物学过程至关重要。蛋白质精氨酸甲基转移酶(PRMTs)的失调与许多病理状况有关。大多数现有的 PRMT 抑制剂显示出有限的特异性和选择性,不加区分地靶向使用 S-腺苷甲硫氨酸作为辅助因子的许多甲基转移酶酶。在这里,我们报告了用于特异性抑制 PRMT1(主要的 I 型酶)的二脒化合物。通过对接、分子动力学和 MM/PBSA 分析以及生化测定来了解这些抑制剂的结合模式和选择性抑制 PRMT1 的分子基础。我们的数据表明,二脒化合物 2,5-双(4-脒基苯基)呋喃(1,呋咱,DB75),一种主要的抑制剂,靶向酶的活性位点,主要与底物竞争,并且对辅助因子非竞争。此外,细胞研究表明,1 是细胞膜可渗透的,能够有效抑制白血病细胞系中细胞内 PRMT1 活性并阻断细胞增殖,而与不同的遗传病变无关。
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